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在小鼠模型中,抗体在针对登革病毒二次感染的异源保护中比免疫细胞发挥着更大的作用。

Antibodies play a greater role than immune cells in heterologous protection against secondary dengue virus infection in a mouse model.

作者信息

Kyle Jennifer L, Balsitis Scott J, Zhang Luhua, Beatty P Robert, Harris Eva

机构信息

Division of Infectious Diseases, School of Public Health, University of California, Berkeley, 1 Barker Hall #424, Berkeley, CA 94720-7354, USA.

出版信息

Virology. 2008 Oct 25;380(2):296-303. doi: 10.1016/j.virol.2008.08.008. Epub 2008 Sep 6.

Abstract

The four serotypes of dengue virus (DENV1-4) are causative agents of dengue fever and dengue hemorrhagic fever/dengue shock syndrome (DHF/DSS). Previous DENV infection is a risk factor for DHF/DSS during subsequent infection by a different serotype. Nonetheless, most primary and secondary DENV infections are asymptomatic. To investigate the possible mechanisms of immune protection in vivo, 129/Pas mice lacking IFN-alpha/beta and -gamma receptors (AG129) were used to model secondary infection using both DENV1-DENV2 and DENV2-DENV4 sequences. At intervals between sequential infections of 4 to 52 weeks, protection against secondary heterologous DENV infection was observed. Passive transfer of DENV-immune serum was protective against replication of heterologous challenge virus in all tissues tested, whereas adoptive transfer of DENV-immune cells significantly protected mice from replication of the challenge virus only when a lower inoculum was administered. These findings are relevant for understanding both natural and vaccine-induced immunity to DENV.

摘要

登革病毒的四种血清型(DENV1 - 4)是登革热和登革出血热/登革休克综合征(DHF/DSS)的病原体。先前的登革病毒感染是后续感染不同血清型时发生DHF/DSS的一个危险因素。尽管如此,大多数原发性和继发性登革病毒感染是无症状的。为了研究体内免疫保护的可能机制,利用缺乏IFN-α/β和 -γ受体的129/Pas小鼠(AG129),采用DENV1 - DENV2和DENV2 - DENV4序列对二次感染进行建模。在连续感染间隔4至52周时,观察到对二次异源登革病毒感染的保护作用。DENV免疫血清的被动转移对所有测试组织中的异源攻击病毒复制具有保护作用,而DENV免疫细胞的过继转移仅在接种量较低时能显著保护小鼠免受攻击病毒的复制。这些发现对于理解登革病毒的天然免疫和疫苗诱导免疫都具有重要意义。

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